4.8 Article

Psilocybin targets a common molecular mechanism for cognitive impairment and increased craving in alcoholism

Journal

SCIENCE ADVANCES
Volume 7, Issue 47, Pages -

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.abh2399

Keywords

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Funding

  1. Bundesministerium fur Bildung und Forschung (BMBF) - ERA-NET program: Psi-Alc [FKZ: 01EW1908]
  2. BMBF-funded SysMedSUDs consortium [01ZX1909A]
  3. Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) [ME 5279/3-1, 402170461-TRR 265 (84)]
  4. European Union [668863-SyBil-AA]

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The study identified a common molecular pathological mechanism for both executive dysfunction and alcohol craving in alcohol-dependent patients, and proposed a personalized mGluR2 mechanism-based intervention strategy for medication development.
Alcohol-dependent patients commonly show impairments in executive functions that facilitate craving and can lead to relapse. However, the molecular mechanisms leading to executive dysfunction in alcoholism are poorly understood, and new effective pharmacological treatments are desired. Here, using a bidirectional neuromodulation approach, we demonstrate a causal link between reduced prefrontal mGluR2 function and both impaired executive control and alcohol craving. A neuron-specific prefrontal mGluR2 knockdown in rats generated a phenotype of reduced cognitive flexibility and excessive alcohol seeking. Conversely, virally restoring prefrontal mGluR2 levels in alcohol-dependent rats rescued these pathological behaviors. In the search for a pharmacological intervention with high translational potential, psilocybin was capable of restoring mGluR2 expression and reducing relapse behavior. Last, we propose a FDG-PET biomarker strategy to identify mGluR2 treatment-responsive individuals. In conclusion, we identified a common molecular pathological mechanism for both executive dysfunction and alcohol craving and provided a personalized mGluR2 mechanism-based intervention strategy for medication development for alcoholism.

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